The Structure of Chloramphenicol Palmitate

of Parke, Davis & Co.] The Structure of Chloramphenicol Palmitate. By William H. Edgerton, V. Harold Maddox and John Controulis. Received June 18, 195...
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THESTRUCTURE OF CHLORAMPHENICOL PALMITATE

Jan. 5, 1955 [CONTRIBUTION FROM

THE

27

PRODUCTS DEVELOPMENT LABORATORIES OF PARKE,DAVIS& Co.]

The Structure of Chloramphenicol Palmitate BY WILLIAMH. EDGERTON, V. HAROLDMADDOX AND

JOHN

CONTROULIS

RECEIVED JUNE 18, 1954 The chromic anhydride oxidation of chloramphenicol palmitate yielded a-dichloroacetamido-p-nitroacrylophenone. Chloramphenicol 1-palmitate was prepared by a procedure involving the stereospecific N -* 01shift of the palmityl moiety.

Chloramphenicol1 has been identified as D-threo2 -dichloroacetamido - 1- ( p - nitrophenyl) - 1,3- propanediol. Chloramphenicol palmitate2 has been developed commercially as a tasteless derivative which; upon ingestion, is hydrolyzed to the active antibiotic. iY02--CH(

OH)CHCHZOCOC~~H,I

I

NHCOCHCIz

I

Since ester formation generally proceeds more readily in the case of primary hydroxyl groups than in the case of secondary hydroxyl groups, it was presumed that the structure of chloramphenicol palmitate was that shown above (I). This structure has been substantiated by the oxidation of chloramphenicol palmitate, the synthesis of the isomeric 1-ester and acylation studies of a series of oxazolines.a This report deals with the oxidation of chloramphenicol palmitate and the preparation of the isomeric chloramphenicol 1-palmitate. Oxidation of chloramphenicol palmitate with the stoichiometric quantity of chromic anhydride in glacial acetic acid a t 50" yielded along with palmitic acid an optically inactive unsaturated ketone, Cl1H8Cl2N204,m.p. 116-117", identical with the dehydration product of a-dichloroacetamido-6hydroxy-p-nitropr~piophenone~ obtained by Osugi.6 O Z N ~- C O C = C H I

I

saturated compound with Osugi's dehydration product. Structure I1 indicates that chloramphenicol palmitate bears the palmityl group on the primary alcoholic carbon atom rather than on the secondary carbon atom. If the original ester had contained the palmityl group on the secondary alcoholic carbon atom, hydrolysis to the alcohol, followed by oxidation and dehydration, would have t o be postulated to explain the formation of 11. I n this case the oxidation of the free primary alcoholic group would have to be very slow to allow the hydrolysis and secondary alcohol oxidation to take place by preference. The preparation of the isomeric chloramphenicol 1-palmitate (VII) was then undertaken to confirm the structure and to determine its chemical as well as pharmacological properties. OH K O ~ ~ - C H I - ~ - C H ~ O I---f I NH2 IV OH IiOz~-&H-cH-cHzOH

I

KHCOC~~HOI

V 0

NHCOCHClz

11 OIN--~-C=YCHO

It

OCC~~HJI S O ~ ~ C H I- ~ H - C H ~ + O H

~HCOCHCI~

NHiHCl

111

The structure I1 has been assigned to the unsaturated compound on the basis of: (1) its ultraviolet spectrum (Amax 266 mp), the isomeric unsaturated aldehyde, structure 111, being expected to absorb in the neighborhood of 310 mp (p-nitrocinnamaldehyde, Xmax 310 mp); (2) its absorption of bromine in carbon tetrachloride; (3) the absence of measurable optical rotation indicating loss of asymmetric centers; (4) its hydrolysis in alcoholic hydrochloric acid yielding the expected p-nitrophenylpropane1,2-dione6; and finally ( 5 ) the identity of the un(1) Chloramphenicol is the generic name of the antibiotic for which the trademark of Parke, Davis and Co. is Chloromycetin. (2) W.H. Edgerton, U. S. Patent 2,662,906 (December 15, 1953); A. J. Glazko, W. H. Edgerton. W. A. Dill and W. R. Lenz, Anlibiotics and Chentofherapy, 3, 234 (1952). (3) W. H. Edgerton and R. L. Hull, t o be published. (4) L. M. Long and H. D. Troutman, THISJOURNAL, 78,481 (1951). (5) K. Osugi, 1. Pharm. SOC.J a p a n , 7 3 , 458 (1952); C. A . , 47, 2749 (1953). (6) V. Petrow, 0.Stephenson and B. Sturgeon, J. Chcm. SOC.,4066 (1953); L. M. Long, Parke, Davis & Co. Laboratories, unpublished

data.

-+

VI 0

N O ~ ~ - I~ H - C H ~ O H SHCOCHC12 VI1

Monoacylation of ~~-threo-%arnino-l-(p-nitrophenyl)-l,3-propanediol (IV) by conventional methods resulted in large amounts of 03,N-dipalmitate, and the Kunz hydrolysis' of this diacyl derivative was unsatisfactory because of the solubility characteristics of the ester. A good yield of the Npalmitate (V) could be obtained, however, by using a ratio of two equivalents of IV to one of acid chloride, and this substance was transformed into the secondary monoester VI by a stereospecific shift. Many instances of such reactions have been re(7) A. Kunz and C. s. Hudson, THISJOURNAL, 48, 1982 (1928)

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WILLIAM H. EDGERTON, v. HAROLD MADDOX AND JOHN CONTROULIS

ported.s The proximal positions of the 2-acylamino and the 1-hydroxyl moieties enables facile formation of a 5-membered ring as an intermediate according to the plausible mechanism postulated by Alberti and co-workers.8 ~ ~ - t h r e o - 2 - h i n o (p - l - nitrophenyl) - 1- 0 - palmityl-1,3-pi opanediol was isolated from the hydrochloride VI by shaking in suspension in an alkaliether system. Although this compound is stable enough to be isolated and characterized,gan 0' .-t S shift occurred when acylation with methyl dichloroacetate was attempted. Acylation of V I was successful with dichloroacetic anhydride in dry benzene. The preparation of D-threo-chloramphenicol 1palmitate was completed essentially as described above with the exception of the dichloroacylation step. D - threo - 2 - Amino - 1- ( p- nitrophenyl) - 1- 0palmityl-1,3-propanediolhydrochloride was acylated in N,N-dimethylformamide with dichloroacetyl chloride. The mechanism of this reaction probably involves the introduction of the dichloroacetyl moiety a t the O 3 position. Neutralization then induces an O 3 + N migration of the dichloroacetyl group rather than the more sluggish palmityl group. The infrared spectra of both D- and DL-l-iSOmerS are characterized by distinctive dichloroacetamido absorption bands a t 5.93 and 5.96 p, respectively. Palmitamido absorption usually occurs a t about 6.06 p . The ultraviolet spectra of the D- and DL1-isomers have peaks which are shifted to 267.5 and 264.5 mp, respectively. The authors wish to thank Dr. George W. Moersch for his advice and Mr. James R. Fisher for his assistance. Infrared and ultraviolet spectra were determined and interpreted by Dr. John M. Vandenbelt, Mr. R. Bruce Scott and Miss Carola Henrich. Microanalytical data were applied by Mr. Charles Childs. Experimentallo Oxidation of Chloramphenicol Palmitate.-To a solution of 17 g. (0.0303 mole) of chloramphenicol palmitate in glacial acetic acid (400 ml.) was added 2 g. (0.0200 mole) of chromium trioxide, dissolved in 2 ml. of water and 5 ml. of glacial acetic acid. The mixture was heated a t 55' for 16 hours. The resulting green solution was concentrated in vacuo a t 55-60' and the residue dissolved in ether and ethyl acetate. After aqueous sodium bicarbonate was added t o neutrality, the organic layer was separated and the aqueous layer extracted with ether-ethyl acetate. The combined organic solutions were dried, concentrated, and the residue triturated with petroleum ether. After filtration, 5.4 g. (68.8%) of yellow crystalline material was obtained, m.p. 114-117'. Recrystallization from petroleum ether-ethyl acetate (1: 1) gave yellow plates, m.p. 116.5-117.5", which decolorized bromine in carbon tetrachloride, gave a positive test with 2,4-dinitrophenylhydrazineas well as a negative Schiff aldehyde test, and had an optical rotation of zero in ethanol ( C 1.3390). Anal. Calcd. for CliH8C12N2O4: C, 43.59; H, 2.66; C1, 23.40. Found: C, 43.86; H,2.98; C1, 23.75. (8) C . G. Alberti, B . Camerino and A. Vercellone, Gaze. chim. d d . , 82, 63 (1952); G. Fodor, J. Kiss and I. Sallay, J. Chcm. SOC.,1858 (1951); S. Ikuma and R. Myokei, J. Pharm. SOC.J a p a n , 72, 957 (1952). (9) This observation is contrary t o the behavior of less bulky groups as noted in reference 8. (10) Melting points are uncorrected.

Vol. 77

The 2,4-dinitrophenylhydrazone melted a t 236-238'. Anal. Calcd. for C17H12C12N607: C, 42.25; H , 2.50. Found: C, 42.56; H, 2.92. A second experiment performed under the same conditions afforded, in addition to the above compound, 5.9 g. of a pale green solid (blue in 2,2,4-trimethylpentane). This material was dissolved in concentrated sulfuric acid to give a deep green solution from which precipitated a waxy, ether soluble solid upon dilution with water. Recrystallization from ether gave 3.1 g. of colorless acid, m.p. 58-60', identified as palmitic acid by the amide (m.p. 102-104°). I n addition, a small quantity (0.16 g.) of p-nitrobenzoic acid was isolated from the aqueous solution. The dehydration of a-dichloroacetamido-p-hydroxy-pnitropropiophenone was carried out by the procedure zf Osugi4 to yield pale yellow crystals, m.p. 116.5-118 , shown to be identical with I1 which was obtained by the chromic anhydride oxidation of I. 1-(p-Nitrophenyl )-propane-1&&one .-A solution of 1 g. in 10 ml. of of a-dichloroacetamido-p-nitroacrylophenone absolute ethanol and 1.5 ml. of concentrated hydrochloric acid was refluxed for four hours. After cooling the solution to 5', 1.2 g. of ammonium chloride was separated by filtration. The filtrate was concentrated, dissolved in 10 ml. of ether, filtered and evaporated t o dryness. The residue was dissolved in 5 mi. of benzene. After treatment with carbon, the clear solution was diluted with 10 ml. of petroleum ether. On standing, crystals were obtained, m.p. 85-87". This material was identical with authentic6 l-(pnitrophenyl)-propane-l,2-dioneas shown by a mixture melting point. ~~-threo-Z-Dichloroacetamido-l-( p-nitrophenyl)-3-O-palmityl-l,3-propanediol.-A solution of 32.3 g. (0.1 mole) of ~~-t~treo-2-dichloracetamido-l(p-nitrophenyl)-1,3-propanediol and 9 ml. of dry pyridine in 50 ml. of N,N-dimethylformamide was stirred while 29 g. of palmityl chloride was added in one portion. After stirring for four hours, the reaction mixture was poured into 400 ml. of cold water acidified with 5 ml. of concentrated hyc$ochloric acid. The crude solid, 55 g. (95'%), m.p. 72-79 , was purified by recrystallization from ethanol; m.p. 90-91 ', yield 65%. Anal. Calcd. for C Z ~ H & ~ Z N Z O C,~ :57.75; H , i.54. Found: C, 57.70; H, 7.74. m-threo-1-( p-Nitrophenyl)-2-palmitamido-l,3-propanediol (V).-A solution of 21.2 g. (0.1 mole) of ~ ~ - t h r e a - 2 amino-l-(p-nitrophenyl)-l,3-propanediol ( V I ) in 250 ml. of N,K-dimethylformamide, which had been dried over anhydrous magnesium sulfate, was stirred rapidly while 13.8 g. (0.05 mole) of palmityl chloride was added dropwise. The reaction mixture was stirred a t room temperature for four hours and poured into 1 1. of water. The mixture was acidified with dilute hydrochloric acid, then washed well with several fresh portions of water. The tan solid, m.p. 6&69', was purified by recrystallization from ethanol or ethyl acetate; m.p. 77-75", yield 65%. Anal. Calcd. for C2J142X205: C, 66.61; H, 9.40. Found: C, 66.69; H, 9.34. D-( - )-threo-1-( p-Nitropheny1)-2-palmitmido-1 ,J-propanediol: yield 55%, m.p. 91", [CtIz6D -24" (2% in ethyl acetate). Anal. Found: C, 66.98; H , 9.21. DL-threo-2-Amino-l-(p-nitrophenyl)-l-O-palmityl-l,3-prOpanediol Hydrochloride (VI).-A solution of 9.0 g. (0.02 mole) of V in SO0 ml. of dry ether was saturated with dry hydrogen chloride gas. After several days, 7.3 g. (76%) of white solid, m.p. 133-135", was isolated. Recrystallization from ethanol or ethyl acetate raised the melting point to 148-149', yield 20%. Anal. Calcd. for C ~ ~ H ~ ~ X Z O C, ~.H 61.64; C ~ : H, 5.86. Found: C, 61.34; H, 8.86. u-( - )-threo-2-Amino-l-(p-nitrophenyl)-l-O-pddtyl-l,3propanediol Hydrochloride: yield 60%, m.p. 167-168', [ c Y ] * ~ D -24.1' (1.33% in ethanol). Anal. Found: C, 62.09; H, 9.21. DL-threo-2-Amino-l-(p-nitropheny~)-l-~-pah~ty~-1,3-prOpanedio1.-A suspension of 3.2 g. of V I in a system of 100 ml. of saturated sodium bicarbonate solution and 200 ml. of ether was shaken until clear. The organic layer was washed with water, dried over anhydrous magnesium sulfate and evaporated; 1.2 g. (41%) of white solid, m.p. 86-87'. Several recq stallizations from ethyl acetate raised the melt-

Jan. 5, 1955

1-METHYL-2-(HYDROXYMETHYL)-PYRROLIDINEAND

-PIPERIDINE ESTERS

29

D-( - )-threo-2-Dichloroacetamido-l-( p-nitropheny1)-1-0palmityl-l,3-propanediol.-A solution of 9 g. (0.0185 mole) of D-0' ester in 75 ml. of dry N,N-dimethylformamide was stirred while 3 g. (0.0204 mole) of dichloroacetyl chloride was added dropwise. After standing for 12 hours, the reac~~-tlrreo-2-D~chloroacetam~do-l-(p-nitrophenyl)-l-O-paltion mixture was poured into ether-sodium carbonate solu-

ing point to 92-93'. The characteristic ester band a t 5.81 p was observed in the infrared spectrum. Anal. Calcd. for CZ~H,IN*O~: C, 66.64; H , 9.40. Found: C, 66.77; H, 9.26. mityl-l,3-propanediol (VU).-A suspension of 6.1 g. (0.0125 mole) of VI in 100 ml. of dry benzene with 3.0 g. (0.0125 mole) of dichloroacetic anhydride was heated a t reflux for 16 hours. After filtration, the filtrate was evaporated in vacuo to a sirup which was taken up in a small volume of isopropyl alcohol and diluted with petroleum ether. After cooling a t 5" overnight, 1.3 g. (19%) of white solid, m.p. 70-75', was recovered. Recrystallization from ethanol The melting point of a raised the melting point t o 88-89'. sample admixed with DL-chloramphenicol palmitate was depressed to 80-82'; El1 185 a t 264.5 mp (in ethanol). Anal. Calcd. for C Z ~ H ~ Z C ~ Z N C,Z O 57.75; ~: H, 7.54. Found: C, 57.52; H, 7.23.

[CONTRIBUTIOX FROM

THE

tion. The ether layer, after shaking, was separated, dried and evaporated in wacuo. The resulting sirup was taken up in hot xylene. Cooling caused the separation of 1.5 g. of the active form of amide V. The filtrate was diluted with petroleum ether and cooled t o cause t$ separation of 1.5 g. (18%) of white solid, m.p. 101-102 . The solid was recrystallized from xylene to a melting point of 105-106'; E+ 179 a t 267.3 mp (in ethanol); -39.5' (2% in ethyl acetate). Anal. Calcd. for Cz7Ha~CltN~Os: C, 57.75; H, 7.54. Found: C, 57.18; H, 7.79. DETROIT,MICHIGAN

COLLEGE OF PHARMACY, UNIVERSITY O F MICHIGAN]

Antispasmodics. XM. Esters of 1-Methyl-2-(hydroxymethy1)-pyrrolidine and 1-Methyl-2- (hydroxymethyl)-piperidine BY F. F. BLICKEAND CHI-JUNG Lu102 RECEIVED MARCH16, 1954 Salts of the diphenylacetate, benzilate, 8-methyltropate and p-aminobenzoate of 1-methyl-2-(hydroxymethy1)-pyrrolidine and also the hydrochloride and methobromide of (l-methyl-2-pyrrolidyl)-methylbenzhydryl ether were prepared. The was synthesized. The hydrochlorides of hydrochloride of the p-aminobenzoate of l-methy1-2-(hydroxymethyl)-piperidine the two basic alcohols underwent Mannich reactions. The pharmacological activity of some of the compounds has been reported.

Since a number of esters of basic alcohols, such as piophenone. 2-(Hydroxymethyl)-piperidine was @-diethylaminoethanol, are active antispasmodics, converted by chloral into the 1-formyl derivative it was of interest to prepare esters of l-methyl-2- which was reduced by lithium aluminum hydride (hydroxymethy1)-pyrrolidine (I) and of 1-methyl-2- to the 1-methyl compound 11. (hydroxymethy1)-piperidine (11). The basic alcoThe diphenylacetate of I was prepared by interhols I and 11 contain the same chain skeleton, action of diphenylacetyl chloride with I. I n order N-C-C-OH, found in the simpler basic alcohol to obtain the benzilate, the alcohol I was converted mentioned above. into l-methyl-2-(chloromethyl)-pyrrolidine (111) In order to obtain the required alcohol I, diethyl which was then allowed to react with benzilic acid glutamate was refluxed in xylene whereby it was according to the Horenstein-Pahlicke p r o c e ~ s . ~ converted into 2-carbethoxy-5-pyrrolidone ; re- Since basic esters of tropic acid, in the form of duction of the pyrrolidone with lithium aluminum salts, are often difficult to obtain in crystalline hydride yielded 2-(hydroxymethy1)-pyrrolidine. i t was decided to employ P-methyltropic acid6 This pyrrolidine, in the form of its hydrochloride, and to treat this acid with I11 by the Horensteinreacted with formaldehyde and acetophenone to Pahlicke procedure. The hydrochloride of the form the hydrochloride of the Mannich base, 8-(2- ester formed, (l-methy1-2-pyrrolidyl)-methyl0hydroxymethylpyrro1idino)-propiophenone. methyltropate, was obtained only as an oil but we When 2- (hydroxymethyl) -pyrrolidine was treated were able to prepare the crystalline methobromide with ~ h l o r a lthe , ~ 1-formyl derivative was obtained; in poor yield. this substance was reduced with lithium aluminum Interaction of the alcohol I with diphenylbromohydride to the desired alcohol I. methane produced (1-methyl-2-pyrrolidyl)-methyl Alcohol I1 was obtained in the following manner. benzhydryl ether. a-Picoline was oxidized to a-picolinic acid which, The hydrochlorides of the p-aminobenzoates of I in the form of the hydrochloride, was hydrogenated and 11 were obtained by catalytic reduction of the to a-pipecolinic acid hydrochloride. After esteri- hydrochlorides of the @-nitroesters. fication and reduction of the ester with lithium The hydrochlorides of the diphenylacetate and aluminum hydride, 2-(hydroxymethy1)-piperidine the benzilate of I were tested a t the Sterling-Winwas obtained. In the form of the hydrochloride, throp Research Institute on the isolated rabbit inthis basic alcohol reacted with formaldehyde and (4) H. Horenstein and H. PBhlicke, B n . , 71, 1644 (1938). (5) Unsuccessful attempts have been made in three different laboraacetophenone to yield the hydrochloride of the to obtain a crystalline salt of 8-diethylaminoethyl tropate. See Mannich base, 8-(2-hydroxymethy1piperidino)-pro-tories 66, 1666 J. von Braun, 0. Braunsdorf and K . Rath, THISJOURNAL, (1) This paper represents part of a dissertation submitted by ChiJung Lu in partial fulfillment of the requirements for the Ph.D. degree in the University of Michigan, 1952. (2) American Foundation for Pharmaceutical Education Fellow. (3) F. F. Blicke and Chi-Jung Lu, THISJOURNAL, T I , 3933 (1952).

(1922); R . R. Buttner and J. W. Cusic, ibid., 66, 262 (1943); H. Raffelson, Dissertation, University of Michigan, 1951, p. 69. (6) This acid can be prepared readily by the use of the Ivanov reaction. See A. W. Weston and R. W. DeNet, THIS JOURNAL, 78, 4221 (1951); F. F. Blicke and H Raffelson, ibid., 74, 1730 (1952).